Scientific Reports (Jul 2017)

Genetic variants including markers from the exome chip and metabolite traits of type 2 diabetes

  • Susanne Jäger,
  • Simone Wahl,
  • Janine Kröger,
  • Sapna Sharma,
  • Per Hoffmann,
  • Anna Floegel,
  • Tobias Pischon,
  • Cornelia Prehn,
  • Jerzy Adamski,
  • Martina Müller-Nurasyid,
  • Melanie Waldenberger,
  • Konstantin Strauch,
  • Annette Peters,
  • Christian Gieger,
  • Karsten Suhre,
  • Harald Grallert,
  • Heiner Boeing,
  • Matthias B. Schulze,
  • Karina Meidtner

DOI
https://doi.org/10.1038/s41598-017-06158-3
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 12

Abstract

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Abstract Diabetes-associated metabolites may aid the identification of new risk variants for type 2 diabetes. Using targeted metabolomics within a subsample of the German EPIC-Potsdam study (n = 2500), we tested previously published SNPs for their association with diabetes-associated metabolites and conducted an additional exploratory analysis using data from the exome chip including replication within 2,692 individuals from the German KORA F4 study. We identified a total of 16 loci associated with diabetes-related metabolite traits, including one novel association between rs499974 (MOGAT2) and a diacyl-phosphatidylcholine ratio (PC aa C40:5/PC aa C38:5). Gene-based tests on all exome chip variants revealed associations between GFRAL and PC aa C42:1/PC aa C42:0, BIN1 and SM (OH) C22:2/SM C18:0 and TFRC and SM (OH) C22:2/SM C16:1). Selecting variants for gene-based tests based on functional annotation identified one additional association between OR51Q1 and hexoses. Among single genetic variants consistently associated with diabetes-related metabolites, two (rs174550 (FADS1), rs3204953 (REV3L)) were significantly associated with type 2 diabetes in large-scale meta-analysis for type 2 diabetes. In conclusion, we identified a novel metabolite locus in single variant analyses and four genes within gene-based tests and confirmed two previously known mGWAS loci which might be relevant for the risk of type 2 diabetes.